@ARTICLE{10.3389/fmicb.2014.00678,
AUTHOR={Davis-Richardson, Austin G. and Ardissone, Alexandria N. and Dias, Raquel and Simell, Ville and Leonard, Michael T. and Kemppainen, Kaisa M. and Drew, Jennifer C. and Schatz, Desmond and Atkinson, Mark A. and Kolaczkowski, Bryan and Ilonen, Jorma and Knip, Mikael and Toppari, Jorma and Nurminen, Noora and Hyöty, Heikki and Veijola, Riitta and Simell, Tuula and Mykkänen, Juha and Simell, Olli and Triplett, Eric W.},
TITLE={Bacteroides dorei dominates gut microbiome prior to autoimmunity in Finnish children at high risk for type 1 diabetes},
JOURNAL={Frontiers in Microbiology},
VOLUME={5},
PAGES={678},
YEAR={2014},
URL={https://www.frontiersin.org/article/10.3389/fmicb.2014.00678},
DOI={10.3389/fmicb.2014.00678},
ISSN={1664-302X},
ABSTRACT={The incidence of the autoimmune disease, type 1 diabetes (T1D), has increased dramatically over the last half century in many developed countries and is particularly high in Finland and other Nordic countries. Along with genetic predisposition, environmental factors are thought to play a critical role in this increase. As with other autoimmune diseases, the gut microbiome is thought to play a potential role in controlling progression to T1D in children with high genetic risk, but we know little about how the gut microbiome develops in children with high genetic risk for T1D. In this study, the early development of the gut microbiomes of 76 children at high genetic risk for T1D was determined using high-throughput 16S rRNA gene sequencing. Stool samples from children born in the same hospital in Turku, Finland were collected at monthly intervals beginning at 4–6 months after birth until 2.2 years of age. Of those 76 children, 29 seroconverted to T1D-related autoimmunity (cases) including 22 who later developed T1D, the remaining 47 subjects remained healthy (controls). While several significant compositional differences in low abundant species prior to seroconversion were found, one highly abundant group composed of two closely related species, Bacteroides dorei and Bacteroides vulgatus, was significantly higher in cases compared to controls prior to seroconversion. Metagenomic sequencing of samples high in the abundance of the B. dorei/vulgatus group before seroconversion, as well as longer 16S rRNA sequencing identified this group as Bacteroides dorei. The abundance of B. dorei peaked at 7.6 months in cases, over 8 months prior to the appearance of the first islet autoantibody, suggesting that early changes in the microbiome may be useful for predicting T1D autoimmunity in genetically susceptible infants. The cause of increased B. dorei abundance in cases is not known but its timing appears to coincide with the introduction of solid food.}
}